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Genetic expansion of Chaperonin-containing TCP-1 (CCT/TRiC) complex subunits yields testis-specific isoforms required for spermatogenesis in planarian flatworms

机译:包含伴侣蛋白的TCP-1(CCT / TRiC)复杂亚基的遗传扩增产生了planar虫扁平虫中精子发生所需的睾丸特异性亚型。

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摘要

Chaperonin-containing Tail-less complex polypeptide 1 (CCT) is a highly conserved, hetero-oligomeric complex that ensures proper folding of actin, tubulin, and regulators of mitosis. Eight subunits (CCT1-8) make up this complex, and every subunit has a homolog expressed in the testes and somatic tissue of the planarian flatworm Schmidtea mediterranea. Gene duplications of four subunits in the genomes of S. mediterranea and other planarian flatworms created paralogs to CCT1, CCT3, CCT4, and CCT8 that are expressed exclusively in the testes. Functional analyses revealed that each CCT subunit expressed in the S. mediterranea soma is essential for homeostatic integrity and survival, whereas sperm elongation defects were observed upon knockdown of each individual testis-specific paralog (Smed-cct1B; Smed-cct3B; Smed-cct4A; and Smed-cct8B), regardless of potential redundancy with paralogs expressed in both testes and soma (Smed-cct1A; Smed-cct3A; Smed-cct4B; and Smed-cct8A). Yet, no detriment was observed in the number of adult somatic stem cells (neoblasts) that maintain differentiated tissue in planarians. Thus, expression of all eight CCT subunits is required to execute the essential functions of the CCT complex. Furthermore, expression of the somatic paralogs in planarian testes is not sufficient to complete spermatogenesis when testis-specific paralogs are knocked down, suggesting that the evolution of chaperonin subunits may drive changes in the development of sperm structure and that correct CCT subunit stoichiometry is crucial for spermiogenesis.
机译:含伴侣蛋白的无尾复合物多肽1(CCT)是高度保守的杂合寡聚复合物,可确保肌动蛋白,微管蛋白和有丝分裂调节剂的正确折叠。八个亚基(CCT1-8)组成了这个复合体,每个亚基都有一个同源基因,在the虫扁虫Schmidtea mediterranea的睾丸和体细胞组织中表达。 S. Mediterraterranea和其他planar虫扁虫基因组中四个亚基的基因重复产生了CCT1,CCT3,CCT4和CCT8的旁系同源物,这些旁系同源物仅在睾丸中表达。功能分析表明,在地中海假单胞菌中表达的每个CCT亚基对于体内稳态和生存都是必不可少的,而在击倒每个睾丸特异性旁系同源物时观察到精子伸长缺陷(Smed-cct1B; Smed-cct3B; Smed-cct4A;和Smed-cct8B),而不考虑在睾丸和躯体(Smed-cct1A; Smed-cct3A; Smed-cct4B;和Smed-cct8A)中表达的同系物的潜在冗余。然而,在涡虫中维持分化组织的成年体干细胞(成神经细胞)的数量未见任何损害。因此,需要表达所有八个CCT亚基来执行CCT复合体的基本功能。此外,当敲除睾丸特异性旁系同源物时,在平面睾丸中体细胞旁系同源物的表达不足以完成精子发生,这表明伴侣蛋白亚基的进化可能驱动精子结构发展的变化,正确的CCT亚基化学计量对于关键是至关重要的。精子发生。

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